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糖蛋白质量控制途径的设计原则。

Design principles for the glycoprotein quality control pathway.

机构信息

Department of Physics, University of California, San Diego, San Diego, California, United States of America.

出版信息

PLoS Comput Biol. 2021 Feb 1;17(2):e1008654. doi: 10.1371/journal.pcbi.1008654. eCollection 2021 Feb.

Abstract

Newly-translated glycoproteins in the endoplasmic reticulum (ER) often undergo cycles of chaperone binding and release in order to assist in folding. Quality control is required to distinguish between proteins that have completed native folding, those that have yet to fold, and those that have misfolded. Using quantitative modeling, we explore how the design of the quality-control pathway modulates its efficiency. Our results show that an energy-consuming cyclic quality-control process, similar to the observed physiological system, outperforms alternative designs. The kinetic parameters that optimize the performance of this system drastically change with protein production levels, while remaining relatively insensitive to the protein folding rate. Adjusting only the degradation rate, while fixing other parameters, allows the pathway to adapt across a range of protein production levels, aligning with in vivo measurements that implicate the release of degradation-associated enzymes as a rapid-response system for perturbations in protein homeostasis. The quantitative models developed here elucidate design principles for effective glycoprotein quality control in the ER, improving our mechanistic understanding of a system crucial to maintaining cellular health.

摘要

内质网中刚翻译的糖蛋白通常经历伴侣蛋白结合和解离的循环,以协助折叠。需要质量控制来区分已经完成天然折叠、尚未折叠和错误折叠的蛋白质。我们使用定量建模来探讨质量控制途径的设计如何调节其效率。我们的结果表明,类似于观察到的生理系统的能量消耗循环质量控制过程,优于替代设计。优化该系统性能的动力学参数随蛋白质产量水平急剧变化,而对蛋白质折叠速率相对不敏感。仅调整降解率,同时固定其他参数,可使途径适应多种蛋白质产量水平,与体内测量结果一致,即降解相关酶的释放是蛋白质动态平衡中扰动的快速反应系统。这里开发的定量模型阐明了内质网中有效糖蛋白质量控制的设计原则,提高了我们对维持细胞健康至关重要的系统的机械理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f689/7877790/675f020780a5/pcbi.1008654.g001.jpg

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